Your search keyword '"Nisenbaum B"' showing total 11 results

1. Abstract P1-07-14: Real-life analysis evaluating >1000 N0/N1mi estrogen receptor (ER)+ breast cancer patients for whom treatment decisions incorporated the 21-gene recurrence score (RS) result: Clinical outcomes with median follow up of > 9 years

Author

Stemmer, SM, primary, Rizel, S, additional, Steiner, M, additional, Geffen, DB, additional, Soussan-Gutman, L, additional, Bareket-Samish, A, additional, McCullough, D, additional, Svedman, C, additional, Nisenbaum, B, additional, Ryvo, L, additional, Peretz, T, additional, Fried, G, additional, Rosengarten, O, additional, Liebermann, N, additional, and Ben Baruch, N, additional

Published

2018

2. First prospectively-designed outcome study in estrogen receptor (ER)+ breast cancer (BC) patients (pts) with N1mi or 1-3 positive nodes in whom treatment decisions in clinical practice incorporated the 21-gene recurrence score (RS) result

Author

Stemmer, S.M., primary, Steiner, M., additional, Rizel, S., additional, Geffen, D., additional, Nisenbaum, B., additional, Peretz, T., additional, Soussan-Gutman, L., additional, Bareket-Samish, A., additional, Isaacs, K., additional, Rosengarten, O., additional, Fried, G., additional, Svedman, C., additional, Shak, S., additional, Liebermann, N., additional, and Ben-Baruch, N., additional

Published

2016

3. Abstract P5-08-02: Real-life analysis evaluating 1594 N0/Nmic breast cancer patients for whom treatment decisions incorporated the 21-gene recurrence score result: 5-year KM estimate for breast cancer specific survival with recurrence score results ≤30 is >98%

Author

Stemmer, SM, primary, Steiner, M, additional, Rizel, S, additional, Soussan-Gutman, L, additional, Geffen, DB, additional, Nisenbaum, B, additional, Ben-Baruch, N, additional, Isaacs, K, additional, Fried, G, additional, Rosengarten, O, additional, Uziely, B, additional, Svedman, C, additional, Rothney, M, additional, Klang, SH, additional, Ryvo, L, additional, Kaufman, B, additional, Evron, E, additional, Zidan, J, additional, Shak, S, additional, and Liebermann, N, additional

Published

2016

4. Abstract P5-20-06: RAD001 (Everolimus) in combination with Letrozole in the treatment of postmenopausal women with estrogen receptor positive Metastatic Breast cancer after failure of hormonal therapy – a phase II study

Author

Safra, T, primary, Kaufman, B, additional, Ben, Baruch N, additional, Kadouri-Sonenfeld, L, additional, Nisenbaum, B, additional, Greenberg, J, additional, Ryvo, L, additional, Yerushalmi, R, additional, and Evron, E, additional

Published

2012

5. First Efficacy Results From the Turandot Phase III Trial Comparing Two Bevacizumab (BEV)-Containing Regimens as First-Line Therapy for HER2-Negative Metastatic Breast Cancer (MBC)

Author

Zielinski, C., primary, Lang, I., additional, Inbar, M., additional, Kahan, Z., additional, Greil, R., additional, Beslija, S., additional, Stemmer, S.M., additional, Kaufman, B., additional, Zvirbule, Z., additional, Steger, G., additional, Melichar, B., additional, Pienkowski, T., additional, Sirbu, D., additional, Petruzelka, L., additional, Eniu, A., additional, Nisenbaum, B., additional, Dank, M., additional, Anghel, R., additional, Messinger, D., additional, and Brodowicz, T., additional

Published

2012

6. Postoperative chemoradiation for resected gastric cancer - is the Macdonald Regimen Tolerable? a retrospective multi-institutional study

Author

Fenig Eyal, Nisenbaum Bella, Pfeffer Raphael M, Karminsky Natalia, Kovel Svetlana, Man Sofia, Lavrenkov Konstantin, Idelevich Efraim, Purim Ofer, Kundel Yulia, Sulkes Aaron, and Brenner Baruch

Subjects

Postoperative chemoradiation, resected gastric cancer, Israeli experience, Medical physics. Medical radiology. Nuclear medicine, R895-920, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Postoperative chemoradiation as per Intergroup-0116 trial ("Macdonald regimen") is considered standard for completely resected high risk gastric cancer. However, many concerns remain with regards to the toxicity of this regimen. To evaluate the safety and tolerability of this regimen in a routine clinical practice setting, we analyzed our experience with its use. As we did not expect a different toxic profile in patients (pts) with positive margins (R1 resection), these were studied together with pts after complete resection (R0). Patients and Methods Postoperative chemoradiation therapy was given according to the original Intergroup-0116 regimen. Overall survival (OS) and disease free survival (DFS) rates were calculated using the Kaplan-Meier method. Comparison of OS and DFS between R0 and R1 pts was done using the log-rank test. Results Between 6/2000 and 12/2007, 166 pts after R0 (129 pts) or R1 (37 pts) resection of locally advanced gastric adenocarcinoma received postoperative chemoradiation; 61% were male and the median age was 63 years (range, 23-86); 78% had T ≥ 3 tumors and 81% had N+ disease; 87% of the pts completed radiotherapy and 54% completed the entire chemoradiation plan; 46.4% had grade ≥ 3 toxicity and 32% were hospitalized at least once for toxicity. Three pts (1.8%) died of toxicity: diarrhea (1), neutropenic sepsis (1) and neutropenic sepsis complicated by small bowel gangrene (1). The most common hematological toxicity was neutropenia, grade ≥ 3 in 30% of pts and complicated by fever in 15%. The most common non-hematological toxicities were nausea, vomiting and diarrhea. With a median follow-up of 51 months (range, 2-100), 62% of the R0 patients remain alive and 61% are free of disease. Median DFS and OS for R0 were not reached. R0 pts had a significantly higher 3-year DFS (60% vs. 29%, p = 0.001) and OS (61% vs. 33%, p = 0.01) compared with R1 pts. Conclusions In our experience, postoperative chemoradiation as per Intergroup-0116 seems to be substantially toxic, with a mortality rate which seems higher than reported in that trial. Efficacy data appears comparable to the original report. Following postoperative chemoradiation, involvement of surgical margins still has a detrimental impact on patient outcome.

Published

2011

7. RAD001 (Everolimus) in combination with Letrozole in the treatment of postmenopausal women with estrogen receptor positive Metastatic Breast cancer after failure of hormonal therapy - a phase II study.

Author

Safra, T., Kaufman, B., Ben, Baruch N., Kadouri-Sonenfeld, L., Nisenbaum, B., Greenberg, J., Ryvo, L., Yerushalmi, R., and Evron, E.

Subjects

*POSTMENOPAUSE, *HORMONE receptors, *HORMONE therapy, *BREAST cancer research, *LETROZOLE, *CANCER in women

Abstract

Background and Objectives: Approximately 70% of postmenopausal women (PMW) present with hormone receptor positive Metastatic Breast cancer (MBC) and there is a need for new treatment modalities after failure of prior endocrine therapy. Activation of the mTOR pathway is a key adaptive change driving endocrine resistance. Pre-clinical and early clinical data suggest synergistic effect between RAD001 (Everolimus, a Novartis mTOR inhibitor) and Letrozole results in more profound effects on proliferation arrest and induction of tumor cell kill. Our objectives are to assess overall response rate (ORR) as well as progression free survival (PFS), overall survival (OS) and safety profile with treatment of Letrozole and RAD001 in PMW with MBC after failure of endocrine therapies. Methods and materials: A multi-center, Israeli phase II open label study evaluating treatment of RAD001 (10 mg daily) combined with Letrozole (2.5 mg daily) in PMW with MBC after recurrence or progression on Tamoxifen and/or Anastrozole and/or Letrozole and/or Fulvestarnt and/or Exemestane. Sixty five patients were enrolled in 7 institutes. This abstract presents data and preliminary results of 24 patients in 2 of the study centers. Median age was 65.5 (54-80) years. Hormonal status were: 50% of the patients had ER+/PR+, 40% ER+/PR- and 10% ER-/PR+. All had MBC with 1 to 3 metastatic sites i.e. bones (90%), liver (30%), lung (12%) and skin (12%). Patients were previously exposed to a median of 1 (1-3) therapy line for MBC, all previously treated with hormonal therapy for MBC and the majority were also exposed to adjuvant hormonal therapy. Results: With a median follow up of 4 months (range 3-12), partial response was observed in 22%, stable disease in 28% and progressive disease in 50% of patients. Median time to progression (TTP) was 4 months (3-11) with 65% still on treatment. Median OS is too early to evaluate (all but 2 are still alive). Grade III bone marrow toxicity was observed in about 5%. Non- hematological toxicities were: grade I fatigue in about 90%, rash and irritation(grade I-II) in about 70%, glucose level, liver function tests, blood cholesterol and triglycerides increased and/or renal function alterations (grade I-III) in about 80%, all the above disappeared after treatment delays or dose reduction, 5% developed non-inflammatory pneumonitis. The 2 most common toxicities were mucositis; 30% grade I and 50% grade II and significant weight loss (5-10% weight reduction) in 90%. Conclusions: Our study shows significant activity with the combination of RAD001 and Letrozole in MBC previously treated several lines of hormonal treatment with an acceptable toxicity. Combining RAD001 with Letrozolein the treatment of MBC, potentially inhibit tumor cell growth\proliferation and act as anti angiogenesis while at the same time potentially preventing the development of Letrozole resistance. Longer follow-up and further evaluation is warranted, additional data will be collected and provided towards the 2012 SABCS. [ABSTRACT FROM AUTHOR]

Published

2012

8. Ten-year clinical outcomes in N0 ER+ breast cancer patients with Recurrence Score-guided therapy.

Author

Stemmer SM, Steiner M, Rizel S, Ben-Baruch N, Uziely B, Jakubowski DM, Baron J, Shak S, Soussan-Gutman L, Bareket-Samish A, Fried G, Rosengarten O, Itay A, Nisenbaum B, Katz D, Leviov M, Tokar M, Liebermann N, and Geffen DB

Abstract

The 21-gene Recurrence Score (RS) assay is a validated prognosticator/predictor of chemotherapy (CT) benefit in early-stage estrogen receptor (ER)-positive breast cancer (BC). Long-term data from real-life clinical practice where treatment was guided by the RS result are lacking. We performed exploratory analysis of the Clalit Health Services (CHS) registry, which included all CHS patients with node-negative ER+ HER2-negative BC who underwent RS testing between 1/2006 and 12/2009 to determine 10-year Kaplan-Meier estimates for distant recurrence/BC-specific mortality (BCSM) in this cohort. The analysis included 1365 patients. Distribution of RS results: RS 0-10, 17.8%; RS 11-25, 62.5%; RS 26-100, 19.7%. Corresponding CT use: 0, 9.4, and 69.9%. Ten-year distant recurrence rates in patients with RS 0-10, 11-25, and 26-100: 2.6% (95% confidence interval [CI], 1.1-6.2%), 6.1% (95% CI, 4.4-8.6%), and 13.1% (95% CI, 9.4-18.3%), respectively ( P  < 0.001); corresponding BCSM rates: 0.7% (95% CI 0.1-5.1%), 2.2% (95% CI, 1.3-3.7%), and 9.5% (95% CI, 6.0-14.9%) ( P  < 0.001). When the analysis included patients treated with endocrine therapy alone (95.5/87.5% of patients with RS 0-10/11-25), 10-year distant recurrence and BCSM rates for RS 0-10 patients were 2.7% (95% CI, 1.1-6.5%) and 0.8% (95% CI, 0.1-5.3%), respectively, and for RS 11-25 patients, 5.7% (95% CI, 3.9-8.3%) and 2.0% (95% CI, 1.1-3.7%), respectively. For RS 11-25 patients, no statistically significant differences were observed in 10-year distant recurrence/BCSM rates between CT-treated and untreated patients; however, this should be interpreted cautiously since the number of events was low and patients were not randomized. In conclusion, in node-negative ER+ HER2-negative BC patients, where treatment decisions in real-life clinical practice incorporated the RS, patients with RS 0-25 (~80% of patients, <10% CT use) had excellent outcomes at 10 years. Patients with RS 26-100 had high distant recurrence risk despite CT use and are candidates for new treatment approaches., Competing Interests: Competing interestsS.M.S. reports receiving grant funding from Teva; receiving travel expenses from Genomic Health, Inc.; conducting research funded by Teva. N.B. reports receiving honoraria from Teva, and serving on the speaker’s bureau of Genomic Health. D.M.J., J.B., and S.S. report being employed by Genomic Health. D.M.J., J.B., and S.S. report having stock ownership in Genomic Health. S.S. reports having intellectual property interest in Genomic Health and a leadership role at Genomic Health. L.S.G. reports being employed by and holding stock options in Teva Pharmaceutical Industries Ltd. A.B.S. reports being a consultant/medical writer for Teva Pharmaceutical Industries Ltd., Genomic Health Inc. (including for the purpose of the current study), Bayer, and Roche. M.S., S.R., B.U., G.F., O.R., A.I., B.N., D.K., M.L., M.T., N.L., and D.B.G. declare no competing interests., (© The Author(s) 2019.)

Published

2019

9. Clinical outcomes in ER+ HER2 -node-positive breast cancer patients who were treated according to the Recurrence Score results: evidence from a large prospectively designed registry.

Author

Stemmer SM, Steiner M, Rizel S, Geffen DB, Nisenbaum B, Peretz T, Soussan-Gutman L, Bareket-Samish A, Isaacs K, Rosengarten O, Fried G, McCullough D, Svedman C, Shak S, Liebermann N, and Ben-Baruch N

Abstract

The Recurrence Score® is increasingly used in node-positive ER+ HER2-negative breast cancer. This retrospective analysis of a prospectively designed registry evaluated treatments/outcomes in node-positive breast cancer patients who were Recurrence Score-tested through Clalit Health Services from 1/2006 through 12/2011 ( N  = 709). Medical records were reviewed to verify treatments/recurrences/survival. Median follow-up, 5.9 years; median age, 62 years; 53.9% grade 2; 69.8% tumors ≤ 2 cm; 84.5% invasive ductal carcinoma; 42.0% N1mi, and 37.2%/15.5%/5.2% with 1/2/3 positive nodes; 53.4% Recurrence Score < 18, 36.4% Recurrence Score 18-30, and 10.2% Recurrence Score ≥ 31. Overall, 26.9% received adjuvant chemotherapy: 7.1%, 39.5%, and 86.1% in the Recurrence Score < 18, 18-30, and ≥ 31 group, respectively. The 5-year Kaplan-Meier estimates for distant recurrence were 3.2%, 6.3%, and 16.9% for these respective groups and the corresponding 5-year breast cancer death estimates were 0.5%, 3.4%, and 5.7%. In Recurrence Score < 18 patients, 5-year distant-recurrence rates for N1mi/1 positive node/2-3 positive nodes were 1.2%/4.4%/5.4%. As patients were not randomized to treatment and treatment decision is heavily influenced by Recurrence Score, analysis of 5-year distant recurrence by chemotherapy use was exploratory and should be interpreted cautiously: In Recurrence Score < 18, recurrence rate was 7.7% in chemotherapy-treated ( n  = 27) and 2.9% in chemotherapy-untreated patients ( n  = 352); P  = 0.245. In Recurrence Score 18-30, recurrence rate in chemotherapy-treated patients ( n  = 102) was significantly lower than in untreated patients ( n  = 156) (1.0% vs. 9.7% P  = 0.019); in Recurrence Score ≤ 25 (the RxPONDER study cutoff), recurrence rate was 2.3% in chemotherapy-treated ( n  = 89) and 4.4% in chemotherapy-untreated patients ( n  = 488); P  = 0.521. In conclusion, our findings support using endocrine therapy alone in ER+ HER2-negative breast cancer patients with micrometastases/1-3 positive nodes and Recurrence Score < 18.

Published

2017

10. Clinical outcomes in patients with node-negative breast cancer treated based on the recurrence score results: evidence from a large prospectively designed registry.

Author

Stemmer SM, Steiner M, Rizel S, Soussan-Gutman L, Ben-Baruch N, Bareket-Samish A, Geffen DB, Nisenbaum B, Isaacs K, Fried G, Rosengarten O, Uziely B, Svedman C, McCullough D, Maddala T, Klang SH, Zidan J, Ryvo L, Kaufman B, Evron E, Karminsky N, Goldberg H, Shak S, and Liebermann N

Abstract

The 21-gene Recurrence Score® (RS) assay is a validated prognostic/predictive tool in ER + early-stage breast cancer. However, clinical outcome data from prospective studies in RS ≥ 11 patients are lacking, as are relevant real-life clinical practice data. In this retrospective analysis of a prospectively designed registry, we evaluated treatments/clinical outcomes in patients undergoing RS-testing through Clalit Health Services. The analysis included N0 ER + HER2-negative breast cancer patients who were RS-tested from 1/2006 through 12/2010. Medical records were reviewed to verify treatments/recurrences/survival. The cohort included 1801 patients (median follow-up, 6.2 years). Median age was 60 years, 50.4% were grade 2 and 81.1% had invasive ductal carcinoma; 48.9% had RS < 18, 40.7% RS 18-30, and 10.4% RS ≥ 31, with chemotherapy use of 1.4, 23.7, and 87.2%, respectively. The 5-year Kaplan-Meier estimates for distant recurrence were 0.8, 3.0, and 8.6%, for patients with RS < 18, RS 18-30 and RS ≥ 31, respectively; the corresponding 5-year Kaplan-Meier estimates for breast cancer death were 0.0, 0.9, and 6.2%. Chemotherapy-untreated patients with RS < 11 ( n  = 304) and 11-25 ( n  = 1037) (TAILORx categorizatio n ) had 5-year Kaplan-Meier estimates for distant recurrence risk/breast cancer death of 1.0%/0.0% and 1.3%/0.4%, respectively. Our results extend those of the prospective TAILORx trial: the 5-year Kaplan-Meier estimates for distant recurrence and breast cancer death rate for the RS < 18 patients were very low supporting the use of endocrine therapy alone. Furthermore, in chemotherapy-untreated patients with RS 11-25 (where TAILORx patients were randomized to chemoendocrine or endocrine therapy alone), 5-year distant recurrence rates were also very low, suggesting that chemotherapy would not have conferred clinically meaningful benefit.

Published

2017

11. Postoperative chemoradiation for resected gastric cancer--is the Macdonald Regimen Tolerable? a retrospective multi-institutional study.

Author

Kundel Y, Purim O, Idelevich E, Lavrenkov K, Man S, Kovel S, Karminsky N, Pfeffer RM, Nisenbaum B, Fenig E, Sulkes A, and Brenner B

Subjects

Adult, Aged, Aged, 80 and over, Chemoradiotherapy methods, Combined Modality Therapy methods, Disease-Free Survival, Female, Fluorouracil administration & dosage, Humans, Leucovorin administration & dosage, Male, Middle Aged, Postoperative Period, Retrospective Studies, Treatment Outcome, Stomach Neoplasms drug therapy, Stomach Neoplasms radiotherapy, Stomach Neoplasms surgery

Abstract

Background: Postoperative chemoradiation as per Intergroup-0116 trial ("Macdonald regimen") is considered standard for completely resected high risk gastric cancer. However, many concerns remain with regards to the toxicity of this regimen. To evaluate the safety and tolerability of this regimen in a routine clinical practice setting, we analyzed our experience with its use. As we did not expect a different toxic profile in patients (pts) with positive margins (R1 resection), these were studied together with pts after complete resection (R0)., Patients and Methods: Postoperative chemoradiation therapy was given according to the original Intergroup-0116 regimen. Overall survival (OS) and disease free survival (DFS) rates were calculated using the Kaplan-Meier method. Comparison of OS and DFS between R0 and R1 pts was done using the log-rank test., Results: Between 6/2000 and 12/2007, 166 pts after R0 (129 pts) or R1 (37 pts) resection of locally advanced gastric adenocarcinoma received postoperative chemoradiation; 61% were male and the median age was 63 years (range, 23-86); 78% had T ≥ 3 tumors and 81% had N+ disease; 87% of the pts completed radiotherapy and 54% completed the entire chemoradiation plan; 46.4% had grade ≥ 3 toxicity and 32% were hospitalized at least once for toxicity. Three pts (1.8%) died of toxicity: diarrhea (1), neutropenic sepsis (1) and neutropenic sepsis complicated by small bowel gangrene (1). The most common hematological toxicity was neutropenia, grade ≥ 3 in 30% of pts and complicated by fever in 15%. The most common non-hematological toxicities were nausea, vomiting and diarrhea. With a median follow-up of 51 months (range, 2-100), 62% of the R0 patients remain alive and 61% are free of disease. Median DFS and OS for R0 were not reached. R0 pts had a significantly higher 3-year DFS (60% vs. 29%, p = 0.001) and OS (61% vs. 33%, p = 0.01) compared with R1 pts., Conclusions: In our experience, postoperative chemoradiation as per Intergroup-0116 seems to be substantially toxic, with a mortality rate which seems higher than reported in that trial. Efficacy data appears comparable to the original report. Following postoperative chemoradiation, involvement of surgical margins still has a detrimental impact on patient outcome.

Published

2011